Apoptosis-Decellularized Peripheral Nerve Scaffold Allows Regeneration across Nerve Gap.

IF 4.7 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2023-01-01 Epub Date: 2022-08-26 DOI:10.1159/000525704
Rebecca A Wachs, Steven M Wellman, Stacy L Porvasnik, Emily H Lakes, R Chase Cornelison, Young Hye Song, Kyle D Allen, Christine E Schmidt
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Abstract

Peripheral nerve injury results in loss of motor and sensory function distal to the nerve injury and is often permanent in nerve gaps longer than 5 cm. Autologous nerve grafts (nerve autografts) utilize patients' own nerve tissue from another part of their body to repair the defect and are the gold standard in care. However, there is a limited autologous tissue supply, size mismatch between donor nerve and injured nerve, and morbidity at the site of nerve donation. Decellularized cadaveric nerve tissue alleviates some of these limitations and has demonstrated success clinically. We previously developed an alternative apoptosis-assisted decellularization process for nerve tissue. This new process may result in an ideal scaffold for peripheral nerve regeneration by gently removing cells and antigens while preserving delicate topographical cues. In addition, the apoptosis-assisted process requires less active processing time and is inexpensive. This study examines the utility of apoptosis-decellularized peripheral nerve scaffolds compared to detergent-decellularized peripheral nerve scaffolds and isograft controls in a rat nerve gap model. Results indicate that, at 8 weeks post-injury, apoptosis-decellularized peripheral nerve scaffolds perform similarly to detergent-decellularized and isograft controls in both functional (muscle weight recovery, gait analysis) and histological measures (neurofilament staining, macrophage infiltration). These new apoptosis-decellularized scaffolds hold great promise to provide a less expensive scaffold for nerve injury repair, with the potential to improve nerve regeneration and functional outcomes compared to current detergent-decellularized scaffolds.

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凋亡去细胞化外周神经支架允许神经间隙再生
周围神经损伤会导致神经损伤远端丧失运动和感觉功能,超过 5 厘米的神经间隙通常是永久性的。自体神经移植(神经自体移植)利用患者身体其他部位的自体神经组织来修复缺损,是治疗的黄金标准。然而,自体组织供应有限,供体神经和损伤神经的大小不匹配,而且神经捐献部位的发病率也很高。去细胞化尸体神经组织缓解了其中一些限制,并在临床上取得了成功。我们之前开发了另一种凋亡辅助神经组织脱细胞工艺。这种新工艺可以温和地去除细胞和抗原,同时保留微妙的地形线索,从而为周围神经再生提供理想的支架。此外,凋亡辅助工艺所需的活性处理时间较短,而且成本低廉。本研究考察了在大鼠神经间隙模型中,凋亡去细胞化外周神经支架与去污剂去细胞化外周神经支架和同种异体移植对照组相比的效用。结果表明,在损伤后 8 周,凋亡脱细胞外周神经支架在功能(肌肉重量恢复、步态分析)和组织学测量(神经丝染色、巨噬细胞浸润)方面的表现与去污剂脱细胞外周神经支架和同种异体移植对照组相似。与目前的去污剂脱细胞支架相比,这些新型凋亡脱细胞支架有望为神经损伤修复提供成本更低的支架,并有可能改善神经再生和功能结果。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
期刊介绍: ACS Applied Bio Materials is an interdisciplinary journal publishing original research covering all aspects of biomaterials and biointerfaces including and beyond the traditional biosensing, biomedical and therapeutic applications. The journal is devoted to reports of new and original experimental and theoretical research of an applied nature that integrates knowledge in the areas of materials, engineering, physics, bioscience, and chemistry into important bio applications. The journal is specifically interested in work that addresses the relationship between structure and function and assesses the stability and degradation of materials under relevant environmental and biological conditions.
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